Activation of activator protein 1 and stress response kinases in epithelial cells colonized by Helicobacter pylori encoding the cag pathogenicity island

Helicobacter pylori interacts with the apical membrane of the gastric epithelium and induces a number of proinflammatory cytokines/chemokines. The subsequent infiltration of macrophages and granulocytes into the mucosa leads to gastric inflammation accompanied by epithelial degeneration. Gastric diseases, e.g peptic ulcer or gastric adenocarcinoma, are more common among people infected with H, pylori strains producing VacA (vacuolating cytotoxin A) and possessing a cog (cytotoxin-associated antigen A) pathogenicity island. For the induction of the cytokine/chemokine genes in response to H. pylori, we studied the signaling leading to the nuclear activation of the early response transcription factor activator protein 1 (AP-1), We found that H. pylori strains carrying the pathogenicity island induce activation of AP-1 and nuclear factor KB, In contrast to the wild type or an isogenic strain without the vacA gene, isogenic H. pylori strains with mutations in certain cog genes revealed only weak AP-1 and nuclear factor KB activation. In respect to the molecular components that direct AP-1 activity, our results indicate a cascade of the cellular stress response kinases c-Jun N-terminal kinase, MAP kinase kinase 4, and p21-activated kinase, and small Rho-GTPases including Rad and Cdc42, which contributes to the activation of proinflammatory cytokines/chemokines induced by H. pylori encoding the cag pathogenicity island.